Literature DB >> 12167173

Combinatorial diversity of fission yeast SCF ubiquitin ligases by homo- and heterooligomeric assemblies of the F-box proteins Pop1p and Pop2p.

Volker Seibert1, Corinna Prohl, Ida Schoultz, Edward Rhee, Rebecca Lopez, Kareem Abderazzaq, Chunshui Zhou, Dieter A Wolf.   

Abstract

BACKGROUND: SCF ubiquitin ligases share the core subunits cullin 1, SKP1, and HRT1/RBX1/ROC1, which associate with different F-box proteins. F-box proteins bind substrates following their phosphorylation upon stimulation of various signaling pathways. Ubiquitin-mediated destruction of the fission yeast cyclin-dependent kinase inhibitor Rum1p depends on two heterooligomerizing F-box proteins, Pop1p and Pop2p. Both proteins interact with the cullin Pcu1p when overexpressed, but it is unknown whether this reflects their co-assembly into bona fide SCF complexes.
RESULTS: We have identified Psh1p and Pip1p, the fission yeast homologues of human SKP1 and HRT1/RBX1/ROC1, and show that both associate with Pop1p, Pop2p, and Pcu1p into a ~500 kDa SCFPop1p-Pop2p complex, which supports polyubiquitylation of Rum1p. Only the F-box of Pop1p is required for SCFPop1p-Pop2p function, while Pop2p seems to be attracted into the complex through binding to Pop1p. Since all SCFPop1p-Pop2p subunits, except for Pop1p, which is exclusively nuclear, localize to both the nucleus and the cytoplasm, the F-box of Pop2p may be critical for the assembly of cytoplasmic SCFPop2p complexes. In support of this notion, we demonstrate individual SCFPop1p and SCFPop2p complexes bearing ubiquitin ligase activity.
CONCLUSION: Our data suggest that distinct homo- and heterooligomeric assemblies of Pop1p and Pop2p generate combinatorial diversity of SCFPop function in fission yeast. Whereas a heterooligomeric SCFPop1p-Pop2p complex mediates polyubiquitylation of Rum1p, homooligomeric SCFPop1p and SCFPop2p complexes may target unknown nuclear and cytoplasmic substrates.

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Year:  2002        PMID: 12167173      PMCID: PMC128837          DOI: 10.1186/1471-2091-3-22

Source DB:  PubMed          Journal:  BMC Biochem        ISSN: 1471-2091            Impact factor:   4.059


  37 in total

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Authors:  R J Deshaies
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Journal:  Nature       Date:  2000-11-16       Impact factor: 49.962

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4.  Regulation of transcription by ubiquitination without proteolysis: Cdc34/SCF(Met30)-mediated inactivation of the transcription factor Met4.

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5.  The spike of S phase cyclin Cig2 expression at the G1-S border in fission yeast requires both APC and SCF ubiquitin ligases.

Authors:  H Yamano; K Kitamura; K Kominami; A Lehmann; S Katayama; T Hunt; T Toda
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6.  SKP2 is required for ubiquitin-mediated degradation of the CDK inhibitor p27.

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10.  The fission yeast COP9/signalosome is involved in cullin modification by ubiquitin-related Ned8p.

Authors:  C Zhou; V Seibert; R Geyer; E Rhee; S Lyapina; G Cope; R J Deshaies; D A Wolf
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  15 in total

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7.  Coupling histone homeostasis to centromere integrity via the ubiquitin-proteasome system.

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8.  F-box-directed CRL complex assembly and regulation by the CSN and CAND1.

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10.  CAND1 controls in vivo dynamics of the cullin 1-RING ubiquitin ligase repertoire.

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